Ko Li-wen, DeTure Michael, Sahara Naruhiko, Chihab Rifki, Yen Shu-Hui
Department of Neuroscience, Mayo Clinic Jacksonville, Jacksonville, FL 32224, USA.
J Mol Neurosci. 2002 Dec;19(3):311-6. doi: 10.1385/jmn:19:3:309.
Filamentous inclusions made of phosphorylated tau constitute a neuropathologic hallmark of Alzheimer's disease and related disorders. Because abnormal accumulation of tau correlates with the decline in cognitive function, it is conceivable that effective intervention at the early stage of tau filament assembly could impede the progression of these neurodegnerative diseases. Cellular models recapitulating the tau aberration are useful for screening and identifying compounds that are capable of interfering with tau aggregation in a cost-effective manner. To develop such cell culture models, we have established from human neuroglioma [H4] and neuronal [BE(2)-M17D] cells conditional transfectants whose transgenic expression of wild-type or mutant tau via inducible expression mechanisms leads to tau aggregation and filament assembly.
由磷酸化tau蛋白构成的丝状内含物是阿尔茨海默病及相关疾病的神经病理学标志。由于tau蛋白的异常积累与认知功能下降相关,因此可以设想,在tau蛋白丝组装的早期阶段进行有效干预可能会阻碍这些神经退行性疾病的进展。重现tau蛋白异常的细胞模型有助于以经济有效的方式筛选和鉴定能够干扰tau蛋白聚集的化合物。为了开发这样的细胞培养模型,我们从人神经胶质瘤[H4]细胞和神经元[BE(2)-M17D]细胞中建立了条件转染细胞系,其通过诱导表达机制对野生型或突变型tau蛋白进行转基因表达,从而导致tau蛋白聚集和丝组装。
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